Chimie pharmaceutique avancée et drug design [ WFARM2501 ]
3.0 crédits ECTS
20.0 h + 10.0 h
2q
Teacher(s) |
Frédérick Raphaël ;
Muccioli Giulio (coordinator) ;
Lambert Didier ;
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Language |
French
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Place of the course |
Bruxelles Woluwe
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Prerequisites |
organic chemistry and medicinal chemistry
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Main themes |
The teacher(s) will discuss first the different techniques allowing the discovery of novel therapeutic targets (lipidomic ' proteomic ' deorphanization), second the methods allowing the identification of hits for a given molecular target (high-throughput screening ; computer assisted de novo drug design); finally the strategies allowing to optimize a hit ('hit to lead') will be discussed (structures-activity relationships ; docking; ')
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Aims |
At the end of the activity the student will be able to
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Interpret, based on what was discussed in class, the results presented in a scientific paper dealing with the development of a novel drug
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Suggest a strategy allowing to identify novel therapeutic targets
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Suggest a strategy allowing to identify novel lead compounds for a given target (enzyme, receptor, ')
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Suggest a strategy allowing to optimize the activity of a drug towards its target
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Evaluation methods |
a written exam and a presentation of a case-study based on a scientific paper
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Content |
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Lipidomics applied to the discovery of novel targets
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Exploring the proteome looking for novel targets : the enzymes ' the receptors
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Proteins as therapeutic target
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Determination of their 3D structure
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Role of protein's 3D models in drug design
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The interest of establishing structure-activity relationships in drug design
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Cycle et année d'étude |
> Master [120] in Pharmacy
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Faculty or entity in charge |
> FARM
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